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学习相关的突触可塑性的性别差异。

Sex differences in synaptic plasticity underlying learning.

机构信息

Department of Anatomy and Neurobiology, University of California, Irvine, CA, USA.

Department of Neurobiology and Behavior, University of California, Irvine, CA, USA.

出版信息

J Neurosci Res. 2023 May;101(5):764-782. doi: 10.1002/jnr.24844. Epub 2021 Apr 12.

DOI:10.1002/jnr.24844
PMID:33847004
原文链接:https://pmc.ncbi.nlm.nih.gov/articles/PMC10337639/
Abstract

Although sex differences in learning behaviors are well documented, sexual dimorphism in the synaptic processes of encoding is only recently appreciated. Studies in male rodents have built upon the discovery of long-term potentiation (LTP), and acceptance of this activity-dependent increase in synaptic strength as a mechanism of encoding, to identify synaptic receptors and signaling activities that coordinate the activity-dependent remodeling of the subsynaptic actin cytoskeleton that is critical for enduring potentiation and memory. These molecular substrates together with other features of LTP, as characterized in males, have provided an explanation for a range of memory phenomena including multiple stages of consolidation, the efficacy of spaced training, and the location of engrams at the level of individual synapses. In the present report, we summarize these findings and describe more recent results from our laboratories showing that in females the same actin regulatory mechanisms are required for hippocampal LTP and memory but, in females only, the engagement of both modulatory receptors such as TrkB and synaptic signaling intermediaries including Src and ERK1/2 requires neuron-derived estrogen and signaling through membrane-associated estrogen receptor α (ERα). Moreover, in association with the additional ERα involvement, females exhibit a higher threshold for hippocampal LTP and spatial learning. We propose that the distinct LTP threshold in females contributes to as yet unappreciated sex differences in information processing and features of learning and memory.

摘要

虽然学习行为中的性别差异有大量记载,但编码过程中的突触变化的性别二态性直到最近才被认识到。雄性啮齿动物的研究建立在长时程增强(LTP)的发现之上,并接受这种依赖于活动的突触强度增加作为编码的机制,以确定协调依赖于活动的亚突触肌动蛋白细胞骨架重塑的突触受体和信号转导活动,这对于持久增强和记忆至关重要。这些分子底物以及在雄性中表征的 LTP 的其他特征,为一系列记忆现象提供了解释,包括多个巩固阶段、间隔训练的效果以及记忆痕迹在单个突触水平上的位置。在本报告中,我们总结了这些发现,并描述了我们实验室的最新结果,表明在雌性中,海马体 LTP 和记忆需要相同的肌动蛋白调节机制,但仅在雌性中,调节性受体(如 TrkB)和包括Src 和 ERK1/2 在内的突触信号转导中介的参与需要神经元衍生的雌激素,并通过膜相关雌激素受体 α(ERα)进行信号转导。此外,与额外的 ERα 参与相关,雌性表现出更高的海马体 LTP 和空间学习阈值。我们提出,女性中独特的 LTP 阈值有助于尚未被认识到的信息处理和学习记忆特征中的性别差异。

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Protein interacting with C-kinase 1 (PICK1) regulates synaptic function and reversal learning in a mouse model for schizophrenia.与C激酶1相互作用的蛋白质(PICK1)在精神分裂症小鼠模型中调节突触功能和逆向学习。
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